Background

Bloodstream infections are associated with significant patient morbidity and mortality. Antimicrobial susceptibility patterns should guide the choice of empiric antimicrobial regimens for patients with bacteremia.

Methods

From January to December of 2002, 82,569 bacterial blood culture isolates were reported to The Surveillance Network (TSN) Database-USA by 268 laboratories. Susceptibility to relevant antibiotic compounds was analyzed using National Committee for Clinical Laboratory Standards guidelines.

Bloodstream infections cause significant morbidity and mortality worldwide and are among the most common healthcare-associated infections [1–6]. It is estimated that 2 million patients per year in the United States acquire infections while in hospitals, approximately 350,000 (10–20%) of these infections involve the bloodstream, and 90,000 (4.5%) are fatal [1, 6, 7]. Advances in medicine, efforts to control medical costs, and incentives for outpatient care have resulted in an increasingly concentrated population of seriously ill patients in hospitals. The incidence of bloodstream infections in patients treated in United States hospitals has been reported to correlate with increasing use of central venous catheters, patient illness (e.g., oncology, burn/trauma, and high-risk nursery), and other predisposing factors, including microorganism, intensive-care unit (ICU) stay, hand washing practices of medical staff, and adherence to infection control practices [1, 5, 6, 8]. Respiratory, genitourinary tract, and intra-abdominal foci are often identifiable sources of bloodstream infections [9]. Bacteremia due to Enterobacteriaceae other than Escherichia coli are associated with increased mortality compared with bloodstream infections due to Gram-positive species [5]. Gram-negative and polymicrobial bacteremia can result in septic shock and mortality is greater with high-grade bacteremia and polymicrobial infection [4, 5, 10]. Efforts need to be extended to prevent and control serious hospital-acquired infections.

The National Nosocomial Infections Surveillance (NNIS) system reported that from 1986 to 1997, coagulase-negative staphylococci and Staphylococcus aureus were the most common organisms isolated from blood cultures of intensive-care unit (ICU) patients, followed by Enterococcus spp., Candida albicans, and Enterobacter spp. [11]. However, only 50% of all positive blood cultures represent true bloodstream infection [5]. Importantly, although coagulase-negative staphylococci are the most frequently isolated organism from blood cultures, they are clinically significant <15% of the time [5]. Coagulase-negative bacteremia is often the result of long-term use of indwelling central and peripheral catheters as well as other prosthetic devices, the ubiquity of these bacteria as normal skin flora, and the ability of these relatively avirulent organisms to adhere to the surface of biomaterials [5]. Previous studies have reported that S. aureus and E. coli are the two most common, clinically significant causes of bloodstream infections in patients in the United States and Europe [4, 5, 12, 13] and that 6–18% of bloodstream infections are polymicrobial [4, 5]. Bacteremia may be transient or indicative of true systemic infection (i.e., sepsis syndrome) with an initial focal source such as the lungs (e.g., pneumonia) or the urinary tract [10].

The potential for antimicrobial resistance is one consideration for physicians when selecting a regimen with which to treat patients. This is particularly important for the treatment of systemic infections as initial antimicrobial chemotherapy is almost invariably empiric and must be based on knowledge of the most frequently isolated etiological agents and their antimicrobial susceptibility patterns. Early initiation of appropriate antimicrobial treatment is critical in decreasing morbidity and mortality among patients with bloodstream infections [14]. The current study reports the prevalence and antimicrobial susceptibility profiles of blood culture isolates from the United States using The Surveillance Network (TSN) Database-USA (Focus Technologies, Herndon, VA).

In the current study, results from the TSN Database-USA from January 1 to December 31, 2002 were used to estimate the prevalence of specific bacterial species as blood culture isolates in the United States and to determine rates of antimicrobial susceptibility for commonly tested agents among the most prevalent species identified. TSN assimilated antimicrobial susceptibility testing and patient demographic data from a network of 268 hospitals in the United States in 2002 [15]. All blood culture isolates were identified at the participating institutions by routine methods in use at each laboratory. Antimicrobial susceptibility testing of patient isolates was conducted onsite by each participating laboratory as a part of their routine diagnostic testing. An inpatient isolate was defined as such by each laboratory participating in TSN. Data from patients in nursing facilities and hospital outpatients were excluded from the current analysis.

Laboratories contributing to TSN databases are all nationally-accredited and are invited to participate in TSN based on factors such as hospital type (e.g., university teaching hospital, community hospital) and antimicrobial susceptibility testing method used as well as the bed size, patient population, and geographic location of the hospital(s) they serve [15]. Only data generated using nationally approved (Food and Drug Administration-approved) testing methods with MIC results interpreted according to NCCLS [16] recommendations are included in TSN Database-USA. In addition, a series of quality-control filters (proprietary critical rule sets) are used to screen susceptibility test results for patterns indicative of testing error; suspect results are removed from analysis for laboratory confirmation. TSN reflects current testing in United States laboratories and is the antimicrobial susceptibility testing data considered when clinical decisions in participating institutions are made. The TSN database presumes the evidence of infection, but no clinical correlates are applied universally. In TSN, any result from the same patient with the same organism identification and the same susceptibility pattern received within five days is considered a repeat culture and is counted only once in the database. In TSN, all isolates are not tested against all agents and variation can be observed for antimicrobial agents of the same class such as expanded-spectrum cephalosporins (ceftriaxone and cefotaxime) and fluoroquinolones (ciprofloxacin and levofloxacin) for which similar in vitro activities have been previously demonstrated.

Table 1 depicts the frequencies of occurrence of the 20 most common bacterial blood culture isolates in the United States in 2002. A total of 82,569 blood culture isolates were reported to TSN Database-USA in 2002. Coagulase-negative staphylococci accounted for 42.0% of all isolates. Six organisms, coagulase-negative staphylococci, Staphylococcus aureus, Enterococcus faecalis, Eschericia coli, Klebsiella pneumoniae, and Enterococcus faecium accounted for >80% of all blood culture isolates. Overall frequencies of isolation were 78.1% gram-positive bacteria and 21.9% gram-negative bacteria.

Table 1

Frequencies of occurrence of bacterial species or groups isolated from blood cultures of hospitalized patients in the United States in 2002

Rank

Bacterial species or group

No. of isolates

% of total no. of isolates

1

Coagulase-negative staphylocci

34,640

42.0

2

S. aureus

13,618

16.5

3

E. faecalis

6,893

8.3

4

E. coli

5,942

7.2

5

K. pneumoniae

2,942

3.6

6

E. faecium

2,873

3.5

7

Viridans group streptococci

2,773

3.4

8

Pseudomonas aeruginosa

2,030

2.5

9

S. pneumoniae

1,901

2.3

10

Enterobacter cloacae

1,550

1.9

11

Serratia marcescens

814

1.0

12

Acinetobacter baumannii

733

0.9

13

Proteus mirabilis

732

0.9

14

Streptococcus agalactiae

626

0.8

15

Klebsiella oxytoca

470

0.6

16

Enterobacter aerogenes

376

0.5

17

Stenotrophomonas maltophilia

256

0.3

18

Citrobacter freundii

245

0.3

19

Streptococcus pyogenes

211

0.3

20

Enterococcus avium

153

0.2

21

Others

2,791

3.4

Total

82,569

100

Table 2 provides susceptibility rates for commonly tested antimicrobial agents for the most frequently isolated bacterial species in 2002. Greater than 99% of oxacillin-susceptible S. aureus isolates and >98% of oxacillin-susceptible coagulase-negative staphylococci isolates were susceptible to amoxicillin-clavulanate, cefotaxime, ceftriaxone, and cefuroxime. Susceptibilities to ciprofloxacin and levofloxacin, respectively were 88.5% and 89.4% for oxacillin-susceptible S. aureus and 82.1% and 82.7% for oxacillin-susceptible coagulase-negative staphylococci. Among viridans group streptococci, ceftriaxone and cefotaxime were equally active based on the susceptibilities of isolates (89.9% and 89.2%, respectively). S. pneumoniae susceptibilities to penicillin and trimethoprim-sulfamethoxazole were <70% while susceptibilities to levofloxacin, amoxicillin-clavulanate, and ceftriaxone all exceeded 97%. Greater than 95% of E. faecalis isolates and 33% of E. faecium isolates from blood were susceptible to vancomycin.

Table 2

In vitro antimicrobial susceptibility testing results for the most common gram-positive and gram-negative bacterial species or groups isolated from blood cultures of hospitalized patients in the United States in 2002

Gram-positive bacteria

Antimicrobial

Total No.

% Susceptible

Oxacillin-susceptible CoNSa

Amoxicillin-clavulanate

1,692

99.8

Cefotaxime

962

99.7

Ceftriaxone

228

98.7

Cefuroxime

131

100

Ciprofloxacin

1,724

82.1

Clindamycin

2,290

91.2

Erythromycin

2,241

59.2

Gentamicin

1,789

95.7

Levofloxacin

1,652

82.7

Ofloxacin

172

72.7

Penicillin

2,106

31.7

Trimethoprim-sulfamethoxazole

2,099

89.2

Vancomycin

2,273

100

Oxacillin-susceptible S. aureus

Amoxicillin-clavulanate

1,854

99.7

Cefotaxime

823

99.6

Ceftriaxone

602

99.8

Cefuroxime

424

99.8

Ciprofloxacin

3,383

88.5

Clindamycin

5,707

93.3

Erythromycin

5,707

69.1

Gentamicin

4,904

97.9

Levofloxacin

3,903

89.4

Ofloxacin

811

84.0

Penicillin

5,532

14.3

Trimethoprim-sulfamethoxazole

4,660

97.8

Vancomycin

5,565

100

E. faecalis

Erythromycin

787

13.2

Levofloxacin

1,793

52.1

Penicillin

2,372

97.1

Vancomycin

3,400

95.4

E. faecium

Erythromycin

421

4.0

Levofloxacin

758

11.3

Penicillin

913

13.3

Vancomycin

1,285

32.9

Viridans group streptococci

Cefotaxime

719

89.2

Ceftriaxone

1,120

89.9

Clindamycin

1,227

89.0

Erythromycin

1,681

46.6

Levofloxacin

661

90.6

Penicillin

2,005

60.0

Vancomycin

1,901

100

S. pneumoniae

Amoxicillin-clavulanate

141

97.2

Cefotaxime

750

96.3

Ceftriaxone

1,149

97.2

Cefuroxime

223

70.9

Clindamycin

634

95.1

Erythromycin

1,023

75.2

Levofloxacin

762

99.5

Ofloxacin

196

95.4

Penicillin

1,345

68.0

Trimethoprim-sulfamethoxazole

675

66.8

Vancomycin

1,190

100

Gram-negative bacteria

Antimicrobial

Total No.

% Susceptible

E coli

Amikacin

3,815

99.1

Amoxicillin-clavulanate

1,417

79.9

Ampicillin

5,192

52.2

Cefazolin

5,167

87.5

Cefepime

2,966

98.3

Cefotaxime

2,967

97.7

Ceftazidime

4,067

96.2

Ceftriaxone

3,820

97.3

Cephalothin

1,879

61.5

Ciprofloxacin

4,633

86.7

Gentamicin

5,171

92.8

Levofloxacin

4,266

86.0

Nitrofurantoin

1,356

97.5

Ofloxacin

456

88.6

Piperacillin-tazobactam

3,887

95.4

Tobramycin

4,414

93.5

Trimethoprim-sulfamethoxazole

5,108

74.8

K. pneumoniae

Amikacin

1,987

97.6

Amoxicillin-clavulanate

867

86.7

Cefazolin

2,576

86.3

Cefepime

1,613

96.5

Cefotaxime

1,502

93.5

Ceftazidime

2,134

88.5

Ceftriaxone

2,104

93.3

Cephalothin

930

75.3

Ciprofloxacin

2,370

90.3

Gentamicin

2,686

91.1

Levofloxacin

2,264

91.4

Nitrofurantoin

835

55.0

Ofloxacin

275

90.2

Piperacillin-tazobactam

1,997

89.9

Tobramycin

2,320

90.7

Trimethoprim-sulfamethoxazole

2,625

87.2

P. aeruginosa

Amikacin

1,563

92.3

Cefepime

1,450

76.7

Ceftazidime

1,764

77.2

Ciprofloxacin

1,734

71.0

Gentamicin

1,858

77.2

Levofloxacin

1,475

68.0

Ofloxacin

199

44.7

Piperacillin-tazobactam

1,484

91.0

Tobramycin

1,708

87.5

aCoNS, coagulase-negative staphylococci

The oxacillin-resistance rate was 49.3% among blood culture isolates of S. aureus and 76.7% among blood culture isolates of coagulase-negative staphylococci (data not shown). Among oxacillin-resistant coagulase-negative staphylococci and S. aureus, susceptibilities were 32.1–32.6% (range) and 7.3–7.6% for fluoroquinolones, respectively, 48.1% and 80.9% for gentamicin, 13.7% and 5.9% for erythromycin, 47.2% and 29.8% for clindamycin, 56.0% and 90.9% for trimethoprim-sulfamethoxazole, and 100% and 100% for vancomycin (data not shown).

For E. coli, ≥ 97% of isolates were susceptible to amikacin, cefepime, cefotaxime, ceftriaxone, and nitrofurantoin; ceftazidime non-susceptibility, a commonly used phenotypic marker for estimating extended-spectrum β-lactamase (ESBL) rates, was 3.8%. For K. pneumoniae, ≥ 90% of isolates were reported susceptible to amikacin, cefepime, cefotaxime, ceftriaxone, ciprofloxacin, levofloxacin, and gentamicin; ceftazidime non-susceptibility was 11.5%. Among P. aeruginosa, amikacin, piperacillin-tazobactam, and tobramycin had the highest rates of susceptibility; however, no agent had susceptibilities ≥ 93%.

The susceptibility of S. aureus to oxacillin from blood culture isolates also varied by <3% for isolates from intensive-care unit (ICU) patients and non-ICU inpatients. The ciprofloxacin susceptibility rate for E. coli was similar for isolates from ICU patients (85.7%) and non-ICU inpatients (86.8%) (Table 3). Similarly, rates of susceptibility to ceftriaxone among E. coli were similar for isolates from ICU patients (96.3%) and non-ICU inpatients (97.5%).

Table 3

In vitro antimicrobial susceptibility of S. aureus to oxacillin and E. coli to ciprofloxacin and ceftriaxone in blood culture isolates from ICU and non-ICU inpatients

Organism

Antimicrobial agent

Inpatient location

No. of isolates

% of isolates susceptible to antimicrobial agent

S. aureus

oxacillin

ICU

1,994

48.1

Non-ICU

9,625

51.2

E. coli

ciprofloxacin

ICU

581

85.7

Non-ICU

4,052

86.8

ceftriaxone

ICU

510

96.3

Non-ICU

3,310

97.5

Combinations of antimicrobial agents are often prescribed as empiric therapy for suspected or laboratory confirmed bloodstream infections. Frequently prescribed combinations include an expanded-spectrum β-lactam or a fluoroquinolone plus an aminoglycoside for the treatment of infections caused by Gram-negative bacilli while combinations of an expanded-spectrum β-lactam or a fluoroquinolone plus vancomycin are often prescribed for suspected or demonstrated infections caused by Gram-positive pathogens. Beta-lactams or fluoroquinolones are associated with aminoglycosides. Table 4 depicts the percentages of isolates susceptible in vitro to one or both antimicrobials in 10 combinations of agents tested against all blood culture isolates reported to TSN Database-USA in 2002. Combining ceftriaxone, ceftazidime, cefepime, piperacillin-tazobactam or ciprofloxacin with gentamicin demonstrated consistent susceptibility rates for each combination (range, 74.8–76.3%). Similarly, combining ceftriaxone, ceftazdime, cefepime, piperacillin-tazobactam or ciprofloxacin with vancomycin demonstrated consistent susceptibility rates for each combination (range, 93.5–96.6%). Combinations including gentamicin demonstrated lower rates of susceptibility by approximately 20% compared with combinations including vancomycin.

Table 4

In vitro susceptibilities of blood culture isolates from hospitalized patients in the United States in 2002 to antimicrobial combinations of a β-lactam or ciprofloxacin plus gentamicin or vancomycin

Antimicrobial Combination

Total no. of isolates tested against one or both of the antimicrobials in the combination

% of isolates susceptible to at least one antimicrobial in the combination

S. aureus and E. coli were identified in previous studies as the two most common blood culture isolates from hospitalized patients in the United States and Europe [4, 5, 12, 13]. In the current study, coagulase-negative staphylococci were the most common blood culture isolates from laboratories in the United States (42.0% of isolates) (Table 1). However, given that coagulase-negative staphylococci isolated from blood cultures are often contaminants (>85% are clinically insignificant) [5] our results agree generally with those previously published. As TSN collects all laboratory data, year-round, it may present a more accurate description of laboratory testing than do centralized point prevalence studies that often exclude the majority of isolates identified by laboratories in a year [12, 13]. Accepting the over-representation of contaminant coagulase-negative staphylococci in clinical laboratories in the United States as observed in TSN Database-USA, the rank order of other pathogens is similar to previous reports describing centralized surveillance studies [12, 13] and hospital review studies [4, 5]. Six organisms, coagulase-negative staphylococci, S. aureus, E. faecalis, E. coli, K. pneumoniae, and E. faecium accounted for >80% of blood culture isolates. Previously, SENTRY has reported similar results for laboratories in the United States, Canada, Latin America, and Europe [12, 13]. In the current study, overall frequencies of isolation were 78.1% gram-positive bacteria and 21.9% gram-negative bacteria.

Oxacillin-resistant S. aureus are extremely important causes of bloodstream infections and evidence has been presented that oxacillin-resistant S. aureus (Table 3) are increasing globally among bloodstream isolates and among isolates from other anatomical sites [12, 17]. Fluoroquinolone resistance has increased in a consistent step-wise manner in the United States and Europe for Enterobacteriaceae, P. aeruginosa, and S. aureus [12, 13, 18, 19]. It is important for clinicians to be updated with current data concerning the susceptibility of commonly prescribed agents such as the fluoroquinolones and also to be aware of trends in longitudinal data. The rates of change in resistance by pathogen and region can help set priorities for focused intervention efforts.

Early clinical suspicion, rigorous diagnostic measures, aggressive initiation of appropriate antimicrobial therapy, comprehensive supportive care, and measures aimed at reversing predisposing causes (e.g., amelioration of an underlying disease, removal of foreign bodies, drainage of abscesses) are the cornerstone of successful management of patients with sepsis syndrome [5, 10]. The selection of antimicrobials to be used for empiric therapy should be based on the local rates of susceptibility and on the site of infection [10]. Early initiation of appropriate antimicrobial treatment is critical in decreasing morbidity and mortality among patients with bloodstream infections due to gram-negative organisms [14]. The initiation of such therapy is almost always empirical, requiring knowledge of the likely pathogen(s) and their usual antimicrobial susceptibility patterns [10, 20]. Combinations of antimicrobial agents are recommended for empiric therapy for patients with bloodstream infections, particularly for those patients with the most adverse prognostic factors [10]. Combination therapy is recommended to cover the broad range of possible pathogens which may be difficult to distinguish clinically, because of the possibility of polymicrobial infections, because they may prevent the emergence of resistance, and because they may have additive or synergistic antimicrobial activity. For the patient with a nosocomial bloodstream infection, initial treatment should consist of an aminoglycoside initially paired with a broad-spectrum β-lactam. Expanded-spectrum cephalosporins are the β-lactam of choice for the non-neutropenic patient because of the greater likelihood of Klebsiella and Staphylococcus infections in these patients [10]. The regimen of an aminoglycoside paired with a penicillin or cephalosporin having antipseudomonal activity is preferred for neutropenic patients, patients with severe chronic obstructive pulmonary disease or bronchiestatis, patients receiving assisted ventilation, and patients with extensive burns [10].

The in vitro potency of ceftriaxone and cefotaxime against E. coli and Klebsiella suggests that single-agent therapy directed against those bacteria may be successful even in severely compromised hosts [10]. The superior pharmacokinetic and pharmacodynamic properties that exist for ceftriaxone when compared with cefotaxime may be a consideration when choosing between these two agents [18]. In the nosocomial setting, extensive data also confirmed the efficacy of ceftriaxone with or without an aminoglycoside in serious Gram-negative infections, pneumonia, spontaneous bacterial peritonitis and as surgical prophylaxis [21]. Ceftriaxone, cefotaxime, and cefepime all have similar indications for pneumonia, skin and skin structure infections, and urinary tract infections; however only ceftriaxone and cefotaxime have an indication for the sepsis syndrome. In the current study, susceptibilities of isolates to one or both agents in combinations of ceftriaxone, ceftazdime, cefepime, piperacillin-tazobactam or ciprofloxacin plus gentamicin were consistent (range, 74.8–76.3%) but lower than similar β-lactam or ciprofloxacin combinations with vancomycin (range, 93.5–96.6%). Ceftazidime, cefepime, imipenem and meropenem appear most active against P. aeruginosa [10].

In conclusion, susceptibilities to some classes of antimicrobials are decreasing, most notably the fluoroquinolones for Enterobacteriaceae and P. aeruginosa. Many older antimicrobials including ceftriaxone continue to retain high rates of susceptibility against many important bacterial pathogens such as those commonly isolated from blood cultures. Against the most clinically important gram-positive species including pneumococci, and gram-negative bacilli such as E. coli (Table 2) susceptibility to ceftriaxone appears to have changed little, if at all, from 1996 to 2002 [18]. While selective pressure for resistance through antimicrobial use is important, infection control practices are critical to limiting the spread of resistant organisms. The life-threatening nature of bacteremia and sepsis underscores the importance of using timely surveillance data to develop rational antimicrobial therapy recommendations and to design strategies to help control antimicrobial resistance [10, 22].

Jarvis WR: The evolving world of healthcare-associated bloodstream infection surveillance and prevention: is your system as good as you think?. Infect Control Hosp Epidemiol. 2002, 23: 236-238.View ArticlePubMedGoogle Scholar

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